Melanoma spread to lymph nodes of the regional basin is a major predictor for melanoma outcome. Since lymph nodes are often resected, they offer the unique opportunity to catch human disseminated melanoma cells (DCCs) before and during metastatic colony formation and to study their interplay with local immune cells. Transcriptome analysis of DCCs identified activation of DCC-derived extracellular vesicle (EVs) production during colony formation, which was paralleled by CD8 T cell exhaustion, strongly suggesting a fundamental role of EVs in DCC-niche communication. We hypothesize that metastatic colony formation is driven by DCC-derived EVs, which modulate phenotype and function of surrounding immune cells and provide growth support to yet pre-colonizing DCC-clones and whose production is activated by oncogenic pathways. The goal of the project is to identify and mechanistically dissect the role of molecular constituents of DCC-derived EVs and oncogenic pathways involved therein.

DFG Programme CRC/Transregios

Subproject of TRR 305:  Striking a moving target: From mechanisms of metastatic colonization to novel systemic therapies

Major Instrumentation Zeta View Win

Instrumentation Group 1950 Partikelzählgeräte und -klassiergeräte (optisch, elektronisch, außer 35

Applicant Institution Universität Regensburg

Project Head Privatdozentin Dr. Melanie Werner-Klein